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Site-specific decreases in DNA methylation in replicating cells following exposure to oxidative stress
[article]
2022
bioRxiv
pre-print
AbstractOxidative stress is a common feature of inflammation-driven cancers, and promotes genomic instability and aggressive tumour phenotypes. It is known that oxidative stress transiently modulates gene expression through the oxidation of transcription factors and associated regulatory proteins. Activated neutrophils produce hypochlorous acid and chloramines that can disrupt DNA methylation via methionine oxidation. The goal of the current study was to determine whether chloramine exposure
doi:10.1101/2022.05.15.491578
fatcat:aguaez62vbhkfe452azqwfofzy